Our Research: Aims

Our Research

Specific Aims
CADASIL/CARASIL: GOM proteome, altered expression of Notch3 targets, and vascular functional deficits
From monogenic to common SVD
Network of genes/proteins driving vessel pathology in CADASIL/CARASIL
Mechanisms underlying functional deficits and brain pathology in CADASIL/CARASIL
Significance of CADASIL/CARASIL-related genes/proteins and disease pathways for common SVD
Methods

Specific Aims

Our overarching hypothesis is that genes encoding the critical pathways underlying CADASIL and CARASIL contribute to the risk of sporadic SVD. We propose that functional defects in resting CBF, autoregulation, NVC, and susceptibility to cortical spreading depression (CSD) contribute to long- term pathological consequences. Our Overall Objective is to identify therapeutic targets for the treatment of SVD.

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Leducq Center Against Small Vessel Disease

Pathogenesis of small vessel disease in the brain

Our Research

Specific Aims

Aim 1: To identify the network of genes/gene products that drive small vessel pathology in CADASIL and CARASIL.

Aim 2: To elucidate the mechanisms linking Notch3 and HtrA1 mutations to the functional deficits and brain pathology in CADASIL and CARASIL.

Aim 3: To assess the contribution of genes of the CADASIL and CARASIL disease pathways to common non-Mendelian SVD.